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Featured researches published by Yoko Nagayama.


Pediatric Allergy and Immunology | 2006

Gender analysis in acute bronchiolitis due to respiratory syncytial virus

Yoko Nagayama; Toshikazu Tsubaki; Shigeru Nakayama; Kyoko Sawada; Kazuko Taguchi; Noriko Tateno; Tsuyoshi Toba

It is reasonable to compare immune reactions between boys and girls because many infections in the early stages are predominant in males. A relationship between immunomodulatory effects of sex hormone surge in boys at early months and infectious diseases is still unclear. We compared clinical features between boys and girls who suffered from wheezing that was initially triggered by acute respiratory syncytial virus (RSV) bronchiolitis. For systemic immune response evaluation, white blood cell (WBC) count, blood eosinophil count, and serum C‐reactive protein (CRP) were measured. For local inflammation evaluation, scores for eosinophils and neutrophils in sputum were evaluated microscopically. Patients consisted of 90 boys and 51 girls. Most children were under 6 months of age. WBC counts and serum CRP levels were significantly increased in girls compared with boys. Blood eosinophilia at the acute stage was rarely observed in children after 6 months of age. For local response evaluation, sputum specimens obtained from 42 boys and 29 girls were microscopically examined. Sputum eosinophil score of 2+ and more was observed in boys (6/42) exclusively. In contrast, sputum neutrophilia was commonly observed in boys and girls. From a follow‐up study, we confirmed that 28 children with RSV bronchiolitis showed wheezing episodes afterwards. However, their blood and sputum eosinophilia during RSV bronchiolitis did not reflect their subsequent wheezing. We speculated that gender‐specific responses to RSV infection might account for male susceptibility. Differences in RSV pathogenecity between boys and girls should be further investigated in terms of asthma progression.


Pediatric Allergy and Immunology | 2001

Analysis of sputum taken from wheezy and asthmatic infants and children, with special reference to respiratory infections

Yoko Nagayama; Toshikazu Tsubaki; Tsuyoshi Toba; Shigeru Nakayama; Ookusu Kiyofumi

Children who are destined to develop asthma are considered to be susceptible to a variety of respiratory pathogens. To elucidate respiratory inflammation among these children, we measured the levels of eosinophil cationic protein (ECP) and tryptase in sputum taken from three different groups of wheezy infants and young children: those with a first wheeze (n = 15); those with recurrent wheeze (n = 27); and those with recurrent wheeze with respiratory distress, namely asthma (n = 56). The numbers of eosinophils or metachromatic cells determined by microscopic analysis of sputum samples were also evaluated in combination with the ECP and tryptase levels. Although neither sputum ECP nor tryptase was a clear discriminative marker that differentiated the three different types of wheezy disease, ECP levels in sputum from the asthma group were significantly higher (2,269.2 ± 6,216.8 ng/g) than those in the recurrent wheezy group (440.3 ± 1,199.8 ng/g) or in the first‐wheeze group (209.0 ± 172.9 ng/g). A similar trend was observed with tryptase levels in sputum, but there were no significant differences among the three groups. Sputum taken from asthmatic children showed a marked accumulation of eosinophils. However, an accumulation of eosinophils in sputum (even in the presence of an elevated level of sputum ECP) was not identified in the asthmatic infants < 1 year of age. An accumlation of eosinophils in sputum was not evident until children became > 1 year old and thereafter the eosinophils rapidly increased in number until the children reached 5 years of age. It was noteworthy that sputa positive for pathogenic bacteria, taken from the 1‐ and 2‐year‐old asthmatic infants, had a tendency to show high levels of ECP but a reduced number of eosinophils. Along with the wheezy episodes induced by viral infection, primarily and occasionally in combination with secondary bacterial infection, eosinophil activation and infiltration may develop. These predestined immune reactions to various pathogens might be associated with triggering the onset of asthma.


Pediatric Allergy and Immunology | 1995

Eosinophils and basophilic cells in sputum and nasal smears taken from infants and young children during acute asthma.

Yoko Nagayama; Y. Odazima; Shigeru Nakayama; Tsuyosi Toba; S. Funabashi

To examine the increase in eosinophils and basophilic cells in the respiratory areas of infants and young children with asthma (n= 111), we analyzed the numbers of eosinophils and basophilic cells in sputum and nasal smears. The number of children with eosinophilia grades of 2+ or greater (> = 11 cells/five fields in x 1000 magnification) in sputum and nasal smears, respectively, in each age group was as follows: 33% and 21% under 1 year, 59% and 64% at 1 year, and 79–80% and 75–78% at 2–3 years. An increased infiltration of basophilic cells according to age was also observed. Infiltration of these cells began earlier than the appearance of IgE antibodies to mite in blood.


Pediatric Allergy and Immunology | 2007

Bacterial colonization in respiratory secretions from acute and recurrent wheezing infants and children

Yoko Nagayama; Toshikazu Tsubaki; Shigeru Nakayama; Kyoko Sawada; Kazuko Taguchi; Tsuyosi Toba; Yoichi Kohno

Lower respiratory tract infection in childhood often results in airway obstruction, characterized by wheezing. However, contribution of bacterial colonization to the wheezy state in children remains unclear. Wheezing and non‐wheezing children requiring hospitalization were classified into three groups: (i) wheezing children having a past history of recurrent wheezing; (ii) wheezing children without such history; and (iii) non‐wheezing children as control subjects. Respiratory secretions as sputum were analyzed microscopically, and cultured. Cultured pathogenic bacterial species in sputum were categorized into two subgroups according to their amounts, i.e., dominant and non‐dominant amounts of colonies. Incidence of bacterial colonization and wheezing were assessed. Hospitalized children were mainly 1‐ to 2‐yr old, and rapidly decreased in number for older ages. Children in the three groups belonged to different clinical entities. Children in the recurrent wheezing group were highly sensitized to mite allergens, and still required hospitalization after 2 yr of age. Incidence of bacterial colonization was similar between the three groups. Dominant and non‐dominant amounts of bacterial colonization were 170/997 (17.1%) and 170/997 (17.1%), respectively, in the recurrent wheezing group; 28/146 (19.2%) and 35/146 (24.0%), respectively, in the acute wheezing group; and 15/56 (26.8%) and 7/56 (12.5%), respectively, in the non‐wheezing group. Regardless of the presence of wheezing, bacterial colonization commonly occurred at a young age in the three groups. In recurrent wheezing children, boys (122/611, 20.0%) carried non‐dominant amounts of bacteria more frequently than girls (48/386, 12.4%) (p < 0.01). Boys showed predominant wheezing and susceptibility to bacterial colonization. Assessment of bacterial colonization allowed us to characterize asthma onset and outgrowth in childhood.


Pediatric Allergy and Immunology | 2006

Age and sex as factors of response to RSV infections among those with previous history of wheezing

Yoko Nagayama; Toshikazu Tsubaki; Kyoko Sawada; Kazuko Taguchi; Shigeru Nakayama; Tsuyoshi Toba

Although enhanced immune reaction caused by the respiratory syncytial virus (RSV) in allergen‐sensitized animal model has been reported, RSV illnesses in children already sensitized or having recurrent wheezing episodes have not been completely studied. In addition, the reason for male dominances in RSV infection at young ages was also inconclusive. Therefore, gender analysis in recurrent wheezing children with RSV infection can shed light on asthma pathogenesis. We studied the clinical features and the laboratory data of RSV infections in children who had recurrent wheezing histories. The subjects with RSV infection consisted of 98 boys and 58 girls. The children under 4 yr of age were 123 (78.8%) in number. Children with pneumonia were 78 and those with febrile episode were 119. Children above 1 yr of age were highly sensitized with mite antigen (75/96, 78.1%). The clinical symptoms and signs differed according to their ages. Children in each age group behaved differently in their immune reaction to RSV. Above all, 3‐yr‐old children deteriorated clinically during acute RSV infection, accompanied by transient elevated C‐reactive protein (CRP) and suppressed blood eosinophil counts. Clinical features differed in several points between boys and girls. In general, the white blood cell count and the CRP levels were higher in girls in every age group. Blood eosinophil counts at the acute illness were significantly higher in boys than girls aged 2 and 3< yr. Age and gender comparison in already sensitized children might suggest a clue to asthma pathogenesis.


Pediatric Pulmonology | 1991

Clinical observations on lower respiratory tract infections with special reference to serum IgE levels

Yoko Nagayama; Nobukiyo Sakurai


Pediatric Pulmonology | 1990

Clinical observations of children with pleuropneumonia due to Mycoplasma pneumoniae

Yoko Nagayama; Nobukiyo Sakurai; Koshi Yamamoto


Allergology International | 1999

Role of bacterial infection in the exacerbation of acute or prolonged asthma attack in children

Yoko Nagayama; Toshikazu Tsubaki; Tsuyoshi Toba; Hiroshi Kawakami; Kiyofumi Okusu


Allergology International | 2004

INTERLEUKIN (IL)-4 AND IL-8 LEVELS IN SPUTUM TAKEN FROM WHEEZY INFANTS AND YOUNG CHILDREN IN RELEVANT TO BACTERIAL COLONIZATION

Yoko Nagayama; Toshikazu Tsubaki; Tsuyoshi Toba; Shigeru Nakayama; Ookusu Kiyofumi


Nihon Shoni Arerugi Gakkaishi. The Japanese Journal of Pediatric Allergy and Clinical Immunology | 1999

RESPIRATORY SYNCYTIAL VIRUS INFECTION AMONG CHILDREN

Yoko Nagayama

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Toshikazu Tsubaki

Boston Children's Hospital

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Shigeru Nakayama

Boston Children's Hospital

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Tsuyoshi Toba

Boston Children's Hospital

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Kazuko Taguchi

Boston Children's Hospital

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Kyoko Sawada

Boston Children's Hospital

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Ookusu Kiyofumi

Boston Children's Hospital

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Tsuyosi Toba

Boston Children's Hospital

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Hiroshi Kawakami

Boston Children's Hospital

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Kiyofumi Okusu

Boston Children's Hospital

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Naoya Sakaguchi

Boston Children's Hospital

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